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JOURNAL READING
Disusun oleh :Dian Muflikhy PutriNIM 112011101076
Dokter Pembimbing:dr. Gogot Suharyanto Sp.OG
SMF ILMU OBSTETRI DAN GINEKOLOGI
RSD DR. SOEBANDI JEMBER
FAKULTAS KEDOKTERAN
UNIVERSITAS JEMBER
2015
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JOURNAL READING
Disusun oleh :Dian Muflikhy PutriNIM 112011101076
Dokter Pembimbing:dr. Gogot Suharyanto Sp.OG
Disusun untuk melaksanakan tugas Kepaniteraan Klinik MadyaSMF Ilmu Obstetri dan Ginekologi di RSD dr. Soebandi
SMF ILMU OBSTETRI DAN GINEKOLOGIRSD DR. SOEBANDI JEMBER
FAKULTAS KEDOKTERAN
UNIVERSITAS JEMBER
2015
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Gynecology & ObstetricsRegmi et al., Gynecol Obstet 2012, 2:4
http://dx.doi.org/10.4172/2161-0932.1000125
Research Article Open Access
Volume 2 • Issue 4 • 1000125Gynecol ObstetISSN:2161-0932 Gynecology an open access journal
Progesterone for Prevention of Recurrent Preterm Labor after ArrestedPreterm Labor- A Randomized Controlled TrialMohan C. Regmi*, Pappu Rijal, Ajay Agrawal and Dhruba Uprety
Department of Obstetrics and Gynecology, BPKIHS, Dharan, Nepal
Abstract
Background: Preterm birth is the major cause of neonatal mortality and morbidity. In developing countries, it’s amajor health hazard. But there are very few evidence based interventions to prevent it. This study focus on preventionof preterm birth.
Methods: A randomized controlled trial was undertaken in BP Koirala Institute of Health Sciences, where 60patients were randomized into group 1 (n=29, weekly intramuscular Progesterone) and group 2 (n=31,no treatment)after the arrest of preterm labor with tocolysis. Their latency period till delivery and recurrence of preterm labor andneonatal outcomes were compared.
Results: There was signi cant reduction in recurrence of preterm labor and increase in latency period inprogesterone group. However neonatal outcomes were similar.
Conclusion: Progesterone is useful in reducing the recurrence of preterm labor in a patient who had pretermlabor.
*Corresponding author: Mohan C. Regmi, Associate Professor, Department ofObstetrics and Gynecology, BPKIHS, Dharan, Nepal, Tel: 9852049414; E-mail:[email protected]
Received June 17, 2012; Accepted July 11, 2012; Published July 17, 2012
Citation: Regmi MC, Rijal P, Agrawal A, Uprety D (2012) Progesterone forPrevention of Recurrent Preterm Labor after Arrested Preterm Labor- A RandomizedControlled Trial. Gynecol Obstet 2:125. doi: 10.4172/2161-0932.1000125
Copyright: © 2012 Regmi MC, et al. This is an open-access article distributedunder the terms of the Creative Commons Attribution License, which permitsunrestricted use, distribution, and reproduction in any medium, provided theoriginal author and source are credited.
Keywords: Progesterone; Preterm labor; ocolysis
IntroductionPreterm birth is the major cause o neonatal mortality and
morbidity [1]. In addition, prematurity is strongly associated withlong-term developmental disabilities, accounting or 1 in 5 childrenwith mental retardation, 1 in 3 children with vision impairment, andalmost hal o children with cerebral palsy. Importantly, low-birth-weight in ants who are spared signicant neonatal morbidity are athigher risk or cardiovascular disease (myocardial in arction, stroke,and hypertension) and diabetes as adults [2]. Te incidence o pretermbirth in developing countries is higher than in developed countries. So,prevention o preterm birth is a public health priority. Pharmacologicaltherapy with a variety o drugs o different categories has been theprimary method o treating acute preterm labour [3]. Patients witharrested preterm labor are at increased risk or recurrence, but tothis point, continued tocolytic treatment with any agent afer arresto acute preterm labor is o questionable value in extending gestationor improving outcome [3,4]. Te efficacy o maintenance tocolytictherapy afer success ul arrest o preterm labor remains controversial.Tis question is not limited to the use o a specic drug as the dataare similar or terbutaline, magnesium sulphate, and calcium channelblockers [3].
Spontaneous preterm birth, that is preterm birth afer laboror rupture o the membranes, represents approximately 75% o allpreterm births [5]. O all treatments evaluated or the preventiono spontaneous preterm birth to date, progestational agents havedemonstrated the greatest promise. Te exact mechanism oprogesterone in the prevention o preterm birth is not known,although progesterone has been shown to prevent the ormation o gap junctions, to have an inhibitory effect on myometrial contractions, andto prevent spontaneous abortion in women in early pregnancy aferexcision o the corpus luteum [6-8]. Progesterone has also been shownto delay parturition in animals [9]. In the last 40 years, progestins havebeen administered to pregnant women or several reasons, includingthreatening miscarriage, recurrent miscarriage, prevention o pretermlabor and luteal support during in vitro ertilization treatment [10-12].
Progesterone is use ul in allowing pregnancy to reach its physiologicterm because at sufficient levels in the myometrium, it blocks theoxytocin effect o prostaglandin F2α and α-adrenergic stimulation and
there ore, increases the α-adrenergic tocolytic response [13]. Naturalprogesterone is ree o any disturbing teratogenic, metabolic, orhemodynamic effects. Tis is not true or certain articial progestagensand -mimetics [14].
In 2003, two widely published double-blind trials, one odaily vaginal progesterone suppositories and the other o weeklyintramuscular injections o 17alpha-hydroxyprogesterone, claimedthat the treatments effectively reduce the incidence o preterm birth inwomen at risk o spontaneous preterm labour [15,16].
In study published in 2007, vaginal progesterone treatmentreduced the rate o preterm birth among women who were at highrisk or preterm birth because o a short cervix [17]. Progesterone haslong been considered important agents in the maintenance o uterinequiescence and has been used extensively in primary and secondaryprevention o preterm labor [15,18].
We there ore, chose this pharmacological agent as the active drugor our study. Tis randomized trial was designed to assess the use
o progesterone therapy in women who presented with symptomso preterm labor in preventing the recurrence o preterm labor andincrease the latency period afer success ul tocolysis.
Methods
Tis randomized controlled trial was per ormed in the Departmento Obstetrics and Gynecology at B.P. Koirala Institute o HealthSciences over the duration o 1.5 years rom 2009 January to June 2010.Te Institutional Ethical Review Board approved this.
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Citation: Regmi MC, Rijal P, Agrawal A, Uprety D (2012) Progesterone for Prevention of Recurrent Preterm Labor after Arrested Preterm Labor- ARandomized Controlled Trial. Gynecol Obstet 2:125. doi: 10.4172/2161-0932.1000125
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Women o 28-34 weeks period o gestation who were admittedto the Obstetrics ward with preterm labor were involved in the studyafer their labor was success ully arrested with tocolytics. Pretermlabor was dened as the simultaneous presence o contractions (> sixcontractions in 30 min) and cervical changes, either shortening and/orsofening or dilation, by manual examination.
Recurrence o preterm labor was dened as recurrence ocontractions within 48 h afer discontinuation o tocolysis and arrest ocontractions. Arrested preterm labor was dened as a 12-h contraction-
ree period afer tocolytic therapy had been discontinued.
Inclusion criteria were singleton pregnancy, intact membranes,no cerclage, cervical dilation o < 2 cm, and the dating o pregnancyconrmed through rst trimester ultrasound scanning or lastmenstrual period. Te cervical dilatation o 2 cm was taken accordingto observation in the institute that > 2cm dilatation was associated withpoor response with tocolysis.
Exclusion criteria included clinical evidence o intra-amnioticin ection or pyelonephritis, medical complications contraindicatingtocolysis, evidence o etal growth retardation, and sonographicevidence o congenital anomalies inconsistent with li e.
At admission, all patients had a haemogram, urine microscopy andculture sensitivity and a high vaginal swab or culture and sensitivity.All patients were given oral tocolytic, with an initial bolus o 30 mgNi edipine ollowed by 10 mg 8 hourly. All patients received antibioticprophylaxis consisting o ablet Azithromycin 500 mg once a day or 5days along with a ve day course o oral Metronidazole. Tey were givensingle course o Betamethasone, consisting o two 12 mg injectionsduring the rst 24 h afer admission. Afer arrested preterm labor wasdiagnosed, the patient was counseled about the study and offered aninstitutional review board-approved in ormed consent document.Patients included in the study were randomized within 24 h o arresto labor. Te random list was prepared with a computer generatednumber list. Odds (progesterone, Group 1) and pairs (control, Group 2)dened treatment allocation (Figure 1). Patients who were enrolled ascases received Hydroxy progesterone Caproate 250 mg intramuscularweekly till 37 completed weeks or earlier i they delivered. Teremaining patients were included as control subjects and receivedno drugs. Tey were discharged or observation in the obstetric clinicweekly. Tey were ollowed up either at clinic or by telephone i they donot ollow at clinic. Te primary outcomes measure were the time untildelivery (latency period) and recurrence o preterm labor within 48 hafer discontinuation o tocolytic treatment and arrest o contraction.Secondary outcome measures were incidence o low birth weight, andperinatal morbidity (respiratory distress syndrome, intraventricularhemorrhage, necrotizing enterocolitis, and proven sepsis) assessed atthe admission to Neonatal Intensive Care Unit (NICU).
Categorical data were tested or signicance with the χ2 and Fisherexact tests. Continuous data were evaluated or normal distribution andtested or signicance with the Student’s t -test. Statistical signicancewas dened as P < 0.05. All patients were included in the analysis.
ResultsTere were total 60 patients at the study duration that ullled the
inclusion criteria and were randomized to receive either progesteroneor no treatment at all. Most o the patients admitted were rom vicinityo the institute in both groups. Only ew o them were (n=8) wereilliterate. None o the patient had history o in ertility. No patients had
history o previous preterm birth. None o the patients were nullipara.Tere was no history o polyhydramnios. All the patients had BishopScore < 3.Both groups were comparable to each other ( able 1).
Tere was signicant increase in latency period in intervention armwith decrease in incidence o recurrent preterm labor ( able 2).
Tere was no difference in neonatal outcome in both groups.
Te birth weight, incidence o respiratory distress syndrome, needo neonatal intensive care unit admission was similar in both groups( able 3).
DiscussionTe study showed signicant reduction in recurrent preterm labor
with the use o progesterone (38% vs. 64%). However neonatal outcomeswere comparable. In 2005, Roberta Mackenzie et al. [19] conducted ameta-analysis evaluating the use o progesterone or women with highrisk o preterm birth. Tree trials were eligible or inclusion. Terewas a signicant reduction in risk o delivery less than 37 weeks withprogestational agents. Tere was no signicant effect on perinatalmortality or serious neonatal morbidity. Te nding was similar to ourstudy. In 2006, a meta-analysis by Aravinthan Coomarasamy et al. [20]evaluated the use o progesterone in prevention o preterm deliveryin high risk patients. A total o nine randomized control trials wereevaluated comprising o about 500 patients. Meta-analyses showedreductions in delivery rates be ore 37 weeks as well as in respiratory
Pa t ents with arrestedpreterm labor (n=60)
Group 1 (17-OHP)n=29, followed t ll
delivery
Group 2 (no Therapy )n=31 followed t ll
delivery
Figure 1: A randomized controlled trial with tocolysis in two different groups.
Variables 17-OHP (n=29) No therapy(n=31) P value*
Age in years(mean) 23.24 ± 3.47 22.81 ± 3.73 0.642
Period of gestation atadmission(weeks) 32.62 ± 1.72 32.90 ± 1.94 0.552
Parity 1.48 1.29
Bishop Score
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Citation: Regmi MC, Rijal P, Agrawal A, Uprety D (2012) Progesterone for Prevention of Recurrent Preterm Labor after Arrested Preterm Labor- ARandomized Controlled Trial. Gynecol Obstet 2:125. doi: 10.4172/2161-0932.1000125
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distress syndrome with progestational agents. Most o the patients hadsome o one or more risk actors or preterm birth prior to pregnancy.Our study had homogenous comparable population prior to onset opreterm labor. A similar study was carried out by Sedigheh BORNAand Noshin SAHABI [21] in ehran in 2004, where progesterone wasgiven to women afer threatened preterm labor in one arm where asanother arm o patients received no treatment. Tere was signicantincrease in mean latency until delivery, decrease in respiratorydistress syndrome, and decrease in low birth weight in progesteronearm group. No signicant differences were ound between recurrentpreterm labor, admission to intensive care unit and neonatal sepsis
or the progesterone and control groups, respectively. Our study hadsignicantly decreased in incidence o recurrent preterm labor inprogesterone arm group.
All the study discussed above except that one by SedighehBORNA and Noshin SAHABI, the comparison was difficult becausein other study it was to prevent the preterm labor with progesterone
with patients already having risk o preterm labor. Our study hadprogesterone started afer the arrest o preterm labor. Te risk presentin our patient was episode o preterm labor arrested by tocolysis. Terewas difference in type o progesterone use and the gestational age atwhich they were recruited. In our study it was bit late (32 weeks).
Te limitation o our study was small sample size and was notcompared with placebo. Tere was no blinding. So selection bias couldnot be reduced.
ConclusionProgesterone are promising agent to reduce the incidence o
recurrent preterm birth afer arrest o preterm labor. Studies withlarger sample size with double blinding as well as earlier recruitment o
patient (at 28-32 weeks) would probably give more convincing results.Acknowledgement
We would extend my sincere thanks to National Health Research Council forsupporting this research. We would like to extend sincere thanks to our instituteand all the participants of the study.
Con ict of Interest
The authors have no potential con ict of interest.
References
1. National Center for Health Statistics, NVSR (2001) Deaths and percentage oftotal deaths for the 10 leading causes of neonatal and postneonatal deaths:United States, 2001.
2. Gluckman PD, Hanson MA (2004) Living with the past: evolution, developmentand patterns of disease. Science 305: 1733-1736.
3. Sanchez-Ramos L, Kaunitz AM, Gaudier FL, Delke I (1999) Ef cacy ofmaintenance therapy after acute tocolysis: a meta-analysis. Am J ObstetGynecol 181: 484-490.
4. Thornton JG (2005) Maintenance tocolysis. BJOG 112 : 118-121.
5. Meis PJ, Goldenberg RL, Mercer BM, Iams JD, Moawad AH, et al. (1998) Thepreterm prediction study: risk factors for indicated preterm births. Maternal-Fetal Medicine Units Network of the National Institute of Child Health andHuman Development. Am J Obstet Gynecol 178: 562-567.
6. Gar eld RE, Kannan MS, Daniel EE (1980) Gap junction formation inmyometrium: control by estrogens, progesterone, and prostaglandins. Am JPhysiol 238: C81-C89.
7. Allen WM, Reynolds SRM (1935) Physiology of the corpus luteum: thecomparative actions of crystalline progestin and crude progestin on uterinemotility in unanesthetized rabbits. Am J Obstet Gynecol 30: 309-318.
8. Csapo AI, Pulkkinen MO, Wiest WG (1973) Effects of luteectomy andprogesterone replacement therapy in early pregnant patients. Am J ObstetGynecol 115: 759-765.
9. Whitely JL, Hartmann PE, Willcox DL, Bryant-Greenwood GD, GreenwoodFC (1990) Initiation of parturition and lactation in the sow: effects of delayingparturition with medroxyprogesterone acetate. J Endocrinol 124: 475-484.
10. Daya S, Gunby J (2004) Luteal phase support in assisted reproduction cycles.
Cochrane Database Syst Rev CD004830.11. Oates-Whitehead RM, Haas DM, Carrier JA (2003) Progestogen for preventing
miscarriage. Cochrane Database Syst Rev CD003511.
12. Friedler S, Raziel A, Schachter M, Strassburger D, Bukovsky I, et al. (1999)Luteal support with micronized progesterone following in-vitro fertilization usinga down-regulation protocol with gonadotrophin releasing hormone agonist: Acomparative study between vaginal and oral administration. Hum Reprod 14:1944-1948.
13. Fuchs AR, Fuchs F (1984) Endocrinology of human parturition: a review. Br JObstet Gynaecol 91: 948-967.
14. Keelan JA, Myatt L, Mitchell MD (1997) Endocrinology and paracrinology ofparturition. In: Elder MG, Lamont RF, Romero R, (Eds) Preterm labor. ChurchillLivingstone, Philadelphia pp: 457-491.
15. da Fonseca EB, Bittar RE, Carvalho MH, Zugaib M (2003) Prophylacticadministration of progesterone by vaginal suppository to reduce the incidenceof spontaneous preterm birth in women at increased risk: A randomizedplacebo-controlled double-blind study. Am J Obstet Gynecol 188: 419-424.
16. Meis PJ, Klebanoff M, Thom E, Dombrowski MP, Sibai B, et al. (2003)Prevention of recurrent preterm delivery by 17 alpha-hydroxyprogesteronecaproate. N Engl J Med 348: 2379-2385.
17. Fonseca EB, Celik E, Parra M, Singh M, Nicolaides KH, et al. (2007)Progesterone and the risk of preterm birth among women with a short cervix. NEngl J Med 357: 462-469.
18. Noblot G, Audra P, Dargent D, Faguer B, Mellier G (1991) The use of micronizedprogesterone in the treatment of menace of preterm delivery. Euro J ObstetGynecol Reprod Biol 40: 203-209.
19. Mackenzie R, Walker M, Armson A, Hannah ME (2006) Progesterone for theprevention of preterm birth among women at increased risk: A systematicreview and meta-analysis of randomized controlled trials. Am J Obstet Gynecol
194: 1234-1242.20. Coomarasamy A, Thangaratinam S, Gee H, Khan KS (2006) Progesterone for
the prevention of preterm birth: A critical evaluation of evidence. Eur J ObstetGynecol Reprod Biol 129: 111-118.
21. Borna S, Sahabi N (2008) Progesterone for maintenance tocolytic therapy afterthreatened preterm labour: A randomised controlled trial. Aust N Z J ObstetGynaecol 48: 58-63.
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Abstrak
Latar belakang : kelahiran preterm merupakan penyebab utama mortalitas dan
morbiditas dari neonatal. Masalah ini menjadi sorotan di negara berkembang.
Tetapi, hanya ada sedikit tindakan medis yang efektif untuk mencegahnya.
Penelitian ini bertujuan pada pencegahan dari kelahiran preterm.
Metode : sebuah kontrol aacak dilakukan di institut ilmu kesehatan BP koirla,
dimana terdapat 60 pasien dimasukkan ke dalam 2 kelompok secara acak ( grup 1,
diberikan progesterone mingguan; grup 2, tidak diberikan perlakuan). Waktu
hingga persalinan terjadi dan kejadian rekurensi dari persalinan preterm dan
keadaan neonatal akan dibandingkan.
Hasil : terdapat hasill signifikan dalam pengurangan kejadian persalinan preterm
dan peningkatan periode latensi dari persalinan dalam kelompok yang diberi
progesteron, namun, kondisi neonatal hampir sama.
Kesimpulan. Progesteron memberikan hasil dalam mengurangi persalinan preterm
pada pasien yag telah mengalami persalinan preterm sebelumnya.
PendahuluanPersalinan preterm adalah penyebab utaama dari mortalitas dan
morbiditas neonatal. Prematuritas berhubugan erat degan disabilitas
perkembangan anak, seperti retardasi mental, gangguan penglihatan, dan cerebral
palsy. Lebih jauh lagi, bayi lahir dengan berat badan rendar lebih beresiko terkena
penyakit kardiovaskuler dan diabetes melitus pada masa dewasa. Insiden
kelahiran preterm pada negara berkembang lebih tinggi dari negara maju. Oleh
karena itu, pencegahan persalinan preterm menjadi masalah kesehatan yang
penting. Terapi farmakologis menjadi metode utama dalam mengobati persalinan
preterm. Pasien dengan persalinan preterm memiiliki tingkat rekurensi yang
tinggi.
Pasien ynag pernah mengalami persalinan prematur memiliki
kesempatan tinggi untuk kekambuhan. Khasiat pemeliharaan tokolitik masih
kontroversial. Begitu juga dengan penggunaan obat terbutalin , magnesium sulfat ,
dan calcium channelblockers
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Kelahiran prematur spontan , yang lahir setelah pecahnya membran,
mewakili sekitar 75 % dari semuakelahiran prematur. Dari semua perawatan
dievaluasi untuk pencegahan kelahiran prematur spontan sampai saat ini , agen
progestasional memiliki potensi besar. Mekanisme yang tepat dari progesteron
dalam pencegahan kelahiran prematur tidak diketahui, meskipun progesteron telah
terbukti mencegah pembentukan gap persimpangan , memiliki efek penghambatan
pada kontraksi miometrium , dan untuk mencegah aborsi spontan pada wanita di
awal kehamilan setelah eksisi korpus luteum. Progesteron juga telah ditunjukkan
untuk menunda proses kelahiran pada hewan. Dalam 40 tahun terakhir , progestin
telah diberikan kepada wanita hamil karena beberapa alasan, abortus iminens,
abortus inibitus, pencegahan persalinan preterm.
Progesteron berguna dalam memungkinkan kehamilan mencapai aterm
pada kadar yang cukup dalam miometrium, bekerja denagn memblok efek
oksitosin prostaglandin F2α dan stimulasi α - adrenergik dan oleh karena itu,
meningkatkan respon tokolitik α - adrenergik. Alam progesteron bebas dari
mengganggu teratogenik , metabolisme , atau efek hemodinamik . Hal ini tidak
berlaku untuk progestagens buatan tertentu dan – mimetics.
Pada tahun 2003 , dua dipublikasikan secara luas percobaan double-
blind, salah satu harian supositoria progesteron vaginal dan lain mingguan
suntikan intramuskular 17alpha - hidroksiprogesteron , mengaku bahwa
perawatan efektif mengurangi kejadian kelahiran prematur di wanita yang berisiko
persalinan prematur spontan.
Dalam studi yang dipublikasikan pada tahun 2007 , pengobatan
progesteron vaginal mengurangi tingkat kelahiran prematur pada wanita yang
berada di tinggi risiko kelahiran prematur karena leher rahim pendek. Progesteron
memiliki lama dianggap agen penting dalam pemeliharaan uterus ketenangan dan
telah digunakan secara luas di primer dan sekunder pencegahan persalinan
prematur.
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Oleh karena itu kita , memilih agen farmakologis ini sebagai obat aktif
untuk penelitian kami . Uji coba secara acak ini dirancang untuk menilai
penggunaanterapi progesteron pada wanita yang disajikan dengan gejalapersalinan
prematur dalam mencegah kekambuhan persalinan prematur dan meningkatkan
masa laten setelah sukses tokolisis.
Metode
Uji coba terkontrol secara acak ini dilakukan di Departemen Obstetri
dan Ginekologi di B.P. Koirala Institut Kesehatan Ilmu selama durasi 1,5 tahun
dari Januari 2009 hingga Juni 2010 . The Institutional Ethical Review Boarddisetujui ini .
Wanita periode 28-34 minggu kehamilan yang dirawat ke bangsal
Obstetri dengan persalinan prematur yang terlibat dalam penelitian ini setelah
kerja mereka berhasil ditangkap dengan tokolitik . prematurtenaga kerja
didefinisikan sebagai keberadaan simultan kontraksi ( > enam kontraksi dalam 30
menit ) dan perubahan serviks , baik shortening dan / atau pelunakan atau
pelebaran , dengan pemeriksaan manual.Kekambuhan persalinan prematur didefinisikan sebagai kambuhnya
kontraksi dalam waktu 48 jam setelah penghentian tokolisis dan penangkapan
kontraksi. Persalinan prematur ditangkap didefinisikan sebagai 12 - h
contractionfree periode setelah terapi tokolitik telah dihentikan.
Kriteria inklusi adalah kehamilan tunggal , membran utuh, ada cerclage ,
dilatasi serviks dari < 2 cm , dan kencan kehamilan dikonfirmasi melalui trimester
pertama ultrasound scanning atau terakhir periode menstruasi. Dilatasi serviks
dari 2 cm diambil sesuai pengamatan di lembaga yang > 2 cm dilatasi dikaitkan
dengan
Tanggapan miskin dengan tokolisis .
Kriteria eksklusi meliputi bukti klinis intra – amnion infeksi atau
pielonefritis, komplikasi medis kontraindikasi tokolisis , bukti retardasi
pertumbuhan janin , dan sonografi bukti anomali kongenital tidak konsisten
dengan kehidupan .
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Saat masuk, semua pasien memiliki haemogram, mikroskop urin dan
sensitivitas budaya dan swab vagina tinggi untuk kultur dan sensitivitas. Semua
pasien diberi tokolitik lisan, dengan bolus awal 30 mg Nifedipine diikuti oleh 10
mg 8 jam. Semua pasien menerima antibiotikprofilaksis terdiri dari Tablet
Azitromisin 500 mg sekali sehari selama 5 hari bersama dengan kursus lima hari
oral Metronidazole. Mereka diberi Tentu saja satu Betametason, yang terdiri dari
dua 12 mg suntikan selama 24 jam pertama setelah masuk. Setelah persalinan
prematur ditangkap adalah didiagnosis, pasien konseling tentang penelitian dan
menawarkan Ulasan kelembagaan dewan disetujui dokumen informed consent.
Pasien dimasukkan dalam penelitian ini diacak dalam waktu 24 jam dari
penangkapan tenaga kerja. Daftar acak disiapkan dengan komputer yang
dihasilkan
daftar nomor. Odds (progesteron, Kelompok 1) dan pasang (kontrol, Kelompok 2)
alokasi pengobatan didefinisikan (Gambar 1). Pasien yang terdaftar sebagai kasus
yang diterima Hydroxy progesteron kaproat 250 mg intramuskular mingguan
sampai 37 minggu selesai atau sebelumnya jika mereka disampaikan. Itu pasien
yang tersisa dimasukkan sebagai subyek kontrol dan menerima tidak ada obat.
Mereka dipulangkan untuk observasi di klinik kebidanan mingguan. Mereka
ditindaklanjuti baik di klinik atau melalui telepon jika mereka lakukan tidak
mengikuti di klinik. Ukuran hasil utama adalah waktu sampai pengiriman (masa
laten) dan kekambuhan persalinan prematur dalam waktu 48 jam setelah
penghentian pengobatan tokolitik dan penangkapan kontraksi. Ukuran hasil
sekunder adalah kejadian berat badan lahir rendah, dan morbiditas perinatal
(sindrom gangguan pernapasan, intraventrikular perdarahan, necrotizing
enterocolitis, dan terbukti sepsis) dinilai pada yang masuk ke Neonatal Intensive
Care Unit (NICU).
Data kategorikal diuji si gnifikansi dengan χ2 dan Fisher tes yang tepat .
Data kontinyu dievaluasi untuk distribusi normal dan diuji signifikansi dengan t -
test pelajar . signifikansi statistik didefinisikan sebagai P < 0,05 . Semua pasien
dimasukkan dalam analisis .
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Ada Total 60 pasien pada durasi studi yang memenuhi kriteria inklusi
dan diacak untuk menerima baik progesteron atau tanpa pengobatan sama sekali .
Sebagian besar pasien mengaku berasal dari sekitarnya dari lembaga pada kedua
kelompok . Hanya sedikit dari mereka yang ( n = 8 ) yang buta huruf . Tak satu
pun dari pasien memiliki riwayat infertilitas . Tidak ada pasiensejarah kelahiran
prematur sebelumnya . Tidak ada pasien yang nulipara. Ada Ada riwayat
polihidramnion . Semua pasien memiliki Bishop Skor < kelompok 3. Baik
sebanding dengan satu sama lain ( Tabel 1).
Gambar 1. Kelompok kontrol acak dengan tokolisis
Variabel 17-OHP (n=29) Tanpaterapi(n=31) Nilai P
Usia (rata-rata) 23.24 ± 3.47 22.81±3.73 0.642
Usia fgestasi 32.62±1.72 32.90±1.94 0.552
Paritas 1.48 1.29
bishop score
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Tidak ada perbedaan dalam hasil neonatal pada kedua kelompok. Berat
lahir, kejadian sindrom gangguan pernapasan , perlu neonatal unit perawatan
intensif tiket masuk adalah serupa pada kedua kelompok ( Tabel 3 ) .
Diskusi
Hasil penelitian menunjukkan penurunan yang signifikan dalam
persalinan prematur berulang dengan penggunaan progesteron ( 38 % vs 64 % ) .
Namun hasil neonatal sebanding . Pada tahun 2005 , Roberta Mackenzie et al .
melakukan meta - analisis mengevaluasi penggunaan progesteron untuk wanita
dengan tinggi risiko kelahiran prematur . Tiga uji coba yang memenuhi syaratuntuk dimasukkan . di sana adalah penurunan yang signifikan dalam risiko
kelahiran kurang dari 37 minggu dengan agen progestasional . Tidak ada efek
yang signifikan pada perinatal mortalitas atau morbiditas neonatal serius . Temuan
ini mirip dengan kami studi . Pada tahun 2006 , sebuah meta - analisis oleh
Aravinthan Coomarasamy et al.mengevaluasi penggunaan progesteron dalam
pencegahan kelahiran prematur pada pasien berisiko tinggi . Sebanyak sembilan
percobaan terkontrol secara acak yang dievaluasi terdiri dari sekitar 500 pasien .Meta - analisis menunjukkan penurunan tarif pengiriman sebelum 37 minggu serta
pernapasansindrom gangguan dengan agen progestasional . Sebagian besar pasien
memiliki beberapa dari satu atau lebih faktor risiko kelahiran prematur sebelum
kehamilan .
Penelitian kami memiliki populasi sebanding homogen sebelum onset persalinan
prematur . Sebuah studi serupa dilakukan oleh Sedigheh BORNA dan Noshin
Sahabi [ 21 ] di Teheran pada tahun 2004 , di mana progesteron adalah diberikan
kepada wanita setelah persalinan prematur mengancam di satu tangan dimana
lengan lain dari pasien tidak menerima pengobatan . Ada signifikanpeningkatan
rata-rata latency sampai melahirkan , penurunan pernapasan distress syndrome ,
dan penurunan berat badan lahir rendah di progesteron kelompok lengan . Tidak
ada perbedaan signifikan yang ditemukan antara berulang persalinan prematur ,
masuk ke unit perawatan intensif dan sepsis neonatal untuk progesteron dan
kelompok kontrol , masing-masing. Penelitian kami memiliki secara signifikan
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menurun pada kejadian persalinan prematur berulang di progesteron lengan
kelompok .
Semua penelitian yang dibahas di atas kecuali bahwa satu per Sedigheh
BORNA dan Noshin sahabi , perbandingan itu sulit karena dalam penelitian lain
adalah untuk mencegah persalinan prematur dengan progesteron dengan pasien
yang sudah memiliki risiko persalinan prematur . Penelitian kami memiliki
progesteron mulai setelah penangkapan persalinan prematur . Saat ini risiko pada
pasien kami adalah episode persalinan prematur ditangkap oleh tokolisis . di sana
perbedaan dalam jenis penggunaan progesteron dan usia kehamilan di yang
mereka direkrut . Dalam penelitian kami itu agak terlambat ( 32 minggu ).
Keterbatasan dari studi kami adalah ukuran sampel yang kecil dan tidak
dibandingkan dengan plasebo . Tidak ada menyilaukan . Jadi bias seleksi bisa
tidak dikurangi .